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首页> 外文期刊>European journal of pain : >Oral nitric-oxide donor glyceryl-trinitrate induces sensitization in spinal cord pain processing in migraineurs: a double-blind, placebo-controlled, cross-over study.
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Oral nitric-oxide donor glyceryl-trinitrate induces sensitization in spinal cord pain processing in migraineurs: a double-blind, placebo-controlled, cross-over study.

机译:口服一氧化氮供体三硝酸甘油酯在偏头痛患者的脊髓疼痛处理中诱导致敏作用:一项双盲,安慰剂对照,交叉研究。

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摘要

Nitric-oxide donor glyceryl-trinitrate (GTN) modulates cerebral and spinal regions that are involved in migraine and pain processing. We hypothesized that in migraineurs, the susceptibility to develop a migraine attack after GTN administration should parallel with an high sensitivity to GTN-induced change in the pain processing at spinal level. We used the temporal summation threshold (TST) of the lower limb nociceptive withdrawal reflex (NWR) and the related pain sensation to study in parallel the time-course of the effect of the GTN administration on the pain processing at spinal level in migraine and healthy subjects. Twenty-eight (21 F; 7M; mean age 34.2 +/- 8.2) migraine and 15 (11 F; 4M; mean age 35.9 +/- 8.9) healthy subjects were recruited in a double-blind, placebo-controlled, cross-over trial. Neurophysiological examinations were carried out before (baseline) and 30', 60', 120', 180' and 240' after GTN (0.9 mg sublingual) or placebo administration during two different sessions. In migraineurs, GTN administration was associated to a significant facilitation in temporal summation of pain (reduced TST and increased painful sensation) 60', 120' and 180' after drug intake when compared to baseline, to placebo condition and to controls after GTN intake. Furthermore, in migraineurs who developed migraine after GTN, a significant facilitation in temporal summation of pain was detected 60', 120' and 180' after drug intake when compared to patients without clinical response. In migraineurs the susceptibility to develop migraine attack after GTN administration seems to be a specific trait of a subgroup of patients linked to a supersensitivity of the pain system to GTN.
机译:一氧化氮供体三硝酸甘油酯(GTN)调节偏头痛和疼痛过程中涉及的大脑和脊髓区域。我们假设,在偏头痛患者中,服用GTN后发生偏头痛的敏感性应该与对GTN引起的脊柱疼痛过程变化的高度敏感性相平行。我们使用下肢伤害感受性退缩反射(NWR)的时间总和阈值(TST)和相关的疼痛感觉,以平行方式研究了GTN给药对偏头痛和健康脊柱水平疼痛处理的影响的时程科目。在双盲,安慰剂对照,交叉对照研究中招募了28名(21 F; 7M;平均年龄34.2 +/- 8.2)偏头痛和15(11 F; 4M;平均年龄35.9 +/- 8.9)健康受试者。过度审判。神经生理学检查是在GTN(0.9 mg舌下)或安慰剂给药之前(基线)和30',60',120',180'和240'(两次)之前进行的。在偏头痛患者中,与基线相比,服用GTN可以显着促进药物摄入后60',120'和180'时的疼痛时间总和(TST减少和疼痛感增加),安慰剂状况和GTN摄入后的对照。此外,与没有临床反应的患者相比,在GTN后发生偏头痛的偏头痛患者中,在服用药物后60',120'和180'发现了暂时性疼痛总和的明显促进。在偏头痛患者中,服用GTN后出现偏头痛的可能性似乎是与疼痛系统对GTN过敏相关的亚组患者的特殊特征。

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